Characterization of HasB, a Serratia marcescens TonB-like protein specifically involved in the haemophore-dependent haem acquisition system

被引:46
作者
Paquelin, A [1 ]
Ghigo, JM [1 ]
Bertin, S [1 ]
Wandersman, C [1 ]
机构
[1] Inst Pasteur, Unite Membranes Bacteriennes, CNRS, URA 2172, F-75724 Paris 15, France
关键词
D O I
10.1046/j.1365-2958.2001.02628.x
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
In Gram-negative bacteria, the TonB-ExbB-ExbD inner membrane multiprotein complex is required for active transport of diverse molecules through the outer membrane. We present evidence that Serratia marcescens, like several other Gram-negative bacteria, has two TonB proteins: the previously characterized TonB(SM), and also HasB, a newly identified component of the has operon that encodes a haemophore-dependent haem acquisition system. This system involves a soluble extracellular protein (the HasA haemophore) that acquires free or haemoprotein-bound haem and presents it to a specific outer membrane haemophore receptor (HasR). TonB(SM) and HasB are significantly similar and can replace each other for haem acquisition. However, TonB(SM), but not HasB, mediates iron acquisition from iron sources other than haem and haemoproteins, showing that HasB and TonB(SM) only display partial redundancy. The reconstitution in Escherichia coli of the S. marcescens Has system demonstrated that haem uptake is dependent on the E. coli ExbB, ExbD and TonB proteins and that HasB is non-functional in E. coli. Nevertheless, a mutation in the HasB transmembrane anchor domain allows it to replace TonB(EC) for haem acquisition. As the change affects a domain involved in specific TonB(EC)-ExbB(EC) interactions, HasB may be unable to interact with ExbB(EC), and the HasB mutation may allow this interaction. In E. coli, the HasB mutant protein was functional for haem uptake but could not complement the other TonB(EC)-dependent functions, such as iron siderophore acquisition, and phage DNA and colicin uptake. Our findings support the emerging hypothesis that TonB homologues are widespread in bacteria, where they may have specific functions in receptor-ligand uptake systems.
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页码:995 / 1005
页数:11
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